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神经内分泌肿瘤和特发性潮红中的血浆P物质:五肽胃泌素刺激试验的价值及生长抑素类似物的作用

Plasma substance-P in neuroendocrine tumors and idiopathic flushing: the value of pentagastrin stimulation tests and the effects of somatostatin analog.

作者信息

Vinik A I, Gonin J, England B G, Jackson T, McLeod M K, Cho K

机构信息

Department of Internal Medicine, University of Michigan Medical Center, Ann Arbor 48109.

出版信息

J Clin Endocrinol Metab. 1990 Jun;70(6):1702-9. doi: 10.1210/jcem-70-6-1702.

Abstract

We examined the role of the potent vasoactive kinin substance-P (SP) in flushing derived from various causes. SP was measured in plasma after acetone/ether extraction using an antiserum directed at the carboxy-terminal 5-11 amino acid region of undecapeptide SP. The antiserum had less than 1% cross-reaction with the other neurokinins, neurokinin-A and neuropeptide-K, that derive from the beta-preprotachykinin gene and share carboxy-terminal residues. Basal and pentagastrin-stimulated SP levels were measured in 22 healthy controls, 11 patients with histologically proven carcinoid tumors, 8 patients with tumors other than carcinoid, and 7 patients with idiopathic flushing (IF). Basal SP levels were less than 10 pg/mL in normal subjects. All patients with midgut carcinoid tumors had SP levels greater than 25 pg/mL, as did 7 of 8 patients with noncarcinoid tumors and 5 of 7 patients with IF. Using 50 pg/mL as the cutoff point, the sensitivity was 63% for detection of a tumor, and 100% of nontumor patients were excluded. Pentagastrin administration uniformly induced flushing and caused a rise in SP levels greater than 150 pg/mL in 5 of 10 patients with carcinoid tumors, 3 of 8 with noncarcinoid tumors, and 0 of 7 with IF, i.e. a SP rise of more than 100 pg/mL suggests a tumor. Administration of somatostatin (150 micrograms) 0.5 h before the pentagastrin abolished flushing in all carcinoid patients and reduced SP levels, but not into the normal range. Long term treatment with SMS significantly reduced flushing and lowered SP levels, but did not restore these to normal. We conclude that 90% of patients with carcinoid/noncarcinoid tumor have raised COOH-terminal SP levels. A basal level above 50 pg/mL or a pentagastrin-stimulated rise of more than 100 pg/mL distinguishes carcinoid from IF. The dissociation between SP concentrations and flushing suggests that SP may not be the only kinin involved in the flushing associated with carcinoid tumors.

摘要

我们研究了强效血管活性激肽物质P(SP)在各种原因引起的潮红中的作用。使用针对十一肽SP羧基末端5 - 11个氨基酸区域的抗血清,在丙酮/乙醚提取后测定血浆中的SP。该抗血清与源自β-前速激肽原基因且共享羧基末端残基的其他神经激肽(神经激肽A和神经肽K)的交叉反应小于1%。在22名健康对照者、11名经组织学证实患有类癌肿瘤的患者、8名患有类癌以外肿瘤的患者以及7名特发性潮红(IF)患者中测量基础和五肽胃泌素刺激后的SP水平。正常受试者的基础SP水平低于10 pg/mL。所有中肠类癌肿瘤患者的SP水平均高于25 pg/mL,8名非类癌肿瘤患者中有7名以及7名IF患者中有5名也是如此。以50 pg/mL作为临界值,检测肿瘤的敏感性为63%,并且100%的非肿瘤患者被排除。给予五肽胃泌素后,10名类癌肿瘤患者中有5名、8名非类癌肿瘤患者中有3名以及7名IF患者中有0名均出现了一致的潮红,并且SP水平升高超过150 pg/mL,即SP升高超过100 pg/mL提示存在肿瘤。在给予五肽胃泌素前0.5小时给予生长抑素(150微克)可消除所有类癌患者的潮红并降低SP水平,但未降至正常范围。长期使用SMS治疗可显著减少潮红并降低SP水平,但未使其恢复正常。我们得出结论,90%的类癌/非类癌肿瘤患者的羧基末端SP水平升高。基础水平高于50 pg/mL或五肽胃泌素刺激后升高超过100 pg/mL可将类癌与IF区分开来。SP浓度与潮红之间的分离表明,SP可能不是参与类癌肿瘤相关潮红的唯一激肽。

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